The I.3.2 developmental mutant has a single nucleotide deletion in the gene centromere identifier.

Cory J Evans ,Ashley Glazier,Alexandra M K Yokomizo,Veronica A Casarez,Norma Y Melendez,Elizabeth Haugan,Sang Nguyen ,Ivana Small,Meaghan Mauger,Morgan Mauger,Randy Hallman,Larry Milshteyn,Lauren A Hehr,Hailee M Pope,Isabella Leifer,David M Pinal,Haley R Guinan,Mark-Brandon M Salinas,Neelufar C Yeoh,Katherine S Acevedo-Vasquez,Skyler Bowen,Matthew Shellin,Shawna N Hunnicutt,Eric J Moore ,Kayla L Bieser,Vanessa I Feliciano,Sierra C Phanphouvong,Emyli J Augustine,Jacob D Kagey

doi:10.17912/micropub.biology.000653

The I.3.2 developmental mutant has a single nucleotide deletion in the gene centromere identifier.

Cory J Evans , Ashley Glazier + Show 27 more

https://doi.org/10.17912/micropub.biology.000653

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Journal: microPublication Biology	Publication Date: Jan 1, 2022
Citations: 2

Affiliation: Loyola Marymount University, Nevada State College, University of Detroit Mercy

#Single Nucleotide Deletion #Non-autonomous Effects + Show 8 more

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Abstract

The mutation I.3.2 was previously identified in a FLP/FRT screen of chromosome 2R for conditional growth regulators. Here we report the phenotypic characterization and genetic mapping of I.3.2 by undergraduate students participating in Fly-CURE, a pedagogical program that teaches the science of genetics through a classroom research experience. We find that creation of I.3.2 cell clones in the developing eye-antennal imaginal disc causes a headless adult phenotype, suggestive of both autonomous and non-autonomous effects on cell growth or viability. We also identify the I.3.2 mutation as a loss-of-function allele of the gene centromere identifier ( cid ), which encodes centromere-specific histone H3 variant critical for chromosomal segregation.

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